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Etiology
The cause of Hyperthyroidism is the presence of thyroid stimulating Immuoglobulin
(Grave's Disease), secondary to the excess of hypothalamic secretion or anterior
pituitary, thyroid tumor hypersecretion. The most common cause of hyperthyroidism
is Grave's disease, an autoimmune disease, the body carelessly forming thyroid
stymulating immunoglobulin (TSI), an antibody targeted by TSH receptors in thyroid
cells.
Epidemiology
Graves' disease (GD) persists as the most frequently-encountered etiology of
hyperthyroidism causing approximately 60-80% of all cases of thyrotoxicosis
worldwide. It is also more frequently found in females with a female-to-male ratio of
8:1 and apparently manifests in the third and fourth decades of life.
Pathophysiology
Thyrotoxicosis is a clinical manifestation of excess thyroid hormones circulating in
the circulation. Hyperthyroidism is a thyrotoxicosis caused by hyperactive thyroid
gland. Whatever the cause of this clinical manifestation is the same, because this
effect is due to the T3 bond with the full T3-core receptor. Stimulated by TSH or TSH-
like substance (TSI, TSAb), the intrinsic autonomy of the gland causes
thyroid increase, seen from radioactive neck-uptake rise. In contrast to the
destruction of glands such as inflammation, inflammation, radiation, cell damage will
occur until the hormones are stored in the follicle out of the blood. It could also be
because the patient is taking excessive thyroid hormones. In this case radioactive
neck-uptake goes down. This distinction is necessary, because generally this second
event, toxicosis without hyperthyroidism, is usually self-limiting disease.
Classification
Hyperthyroidism can arise spontaneously or due to excessive intake of thyroid
hormones. There are two types of spontaneous hyperthyroidism most commonly
encountered are Graves' disease and nodular toxic goiter. In Graves' disease there
are two main groups of thyroid and extratiroidal features, and both may be invisible.
Thyroidal features of goitre due to thyroid gland hyperplasia, and hyperthyroidism
due to excessive thyroid hormone secretion. Patients complain, shudder, can not
stand the heat, more sweat when hot, moist, heavy skin
body decreases, often accompanied by increased appetite, palpitations and
tachycardia, diarrhea, and muscle weakness and atrophy. Extratiroidal
manifestations of ophthalmopathy are characterized by bulging eyes, widened
palpebral fissures, diminished winks, lig lag, and failure of convergence. Toxic
nodular goiter, more common in elderly patients as a chronic nodular goiter
complication, is a milder manifestation of Graves' disease.
Diagnosis of hyperthyroidism
To distinguish between hyperthyroidism and other causes of thyrotoxicosis, a
radioactive iodine uptake (RAIU) should be performed. Hyperthyroidism has high
RAIU while the other etiologies have low or near absent radioactive iodine uptake.
The assessment of hyperthyroidism manifestations, and especially potential
cardiovascular and neuromuscular complications, is essential to formulating an
appropriate treatment plan.
Clinical evaluation
Biochemical evaluation of TSH and thyroid hormones is the most important initial
diagnostic test for individuals suspected of hyperthyroidism/thyrotoxic crisis based on
clinical manifestations. When there is inconsistency among the clinical signs and
symptoms, or when clinical manifestations are subtle, or confirmatory biochemical
testing is not readily accessible, it may be helpful to use a diagnostic index called the
Wayne' s index. This is a scoring system that has been developed since 1972 to help
improve the diagnostic accuracy of clinical assessment.
Biochemical evaluation
Serum TSH
Serum TSH measurement has the highest sensitivity and specificity of any single
blood test and is used as an initial screening test for hyperthyroidism. In
hyperthyroidism, serum TSH will be less than 0.01 mU/L or even undetectable.
To assess the severity of the condition and to improve diagnostic accuracy, both TSH
and free T4 levels should be assessed at the time of the initial evaluation. In overt
hyperthyroidism, usually both serum free T4 and T3 estimates are elevated, and
serum TSH is < 0.01 mU/L or undetectable. In milder hyperthyroidism, serum T4 and
free T4 estimates can be normal, only serum T3 may be elevated, and serum TSH
will be less than 0.01 mU/L (or undetectable) – called T3 thyrotoxicosis. Assays for
estimating free T3 are less widely-validated than those for free T4, and therefore
measurement of total T3 is frequently preferred in clinical practice. Subclinical
hyperthyroidism is defined as a normal serum free T4 estimate and normal total T3
or free T3 estimate, with subnormal serum TSH concentration.
This approach is utilized when a thyroid scan and uptake are unavailable or
contraindicated (e.g., during pregnancy and lactation).
Ultrasonography (USG)
USG is performed with the patient in the supine position and the neck hyper-
extended. USG can detect thyroid lobes or lesions as small as 2 mm. It can
distinguish solid nodules from simple and complex cysts. It can estimate thyroid size,
give a rough estimate of tissue density, show vascular flow and velocity and aid in
placing a needle for diagnostic purpose. Doppler studies may be added while
executing ultrasonography.
Management
The principle of treatment depends on the etiology of thyrotoxicosis, the age of the
patient, the natural history of the disease, the availability of treatment modality, the
patient's situation, the risk of treatment, and so on.
Treatment of thyrotoxicosis is grouped into:
1. Tirostatiska: tioimidazole derivative group (CBZ, 5 mg carbimazole, MTZ,
metimazole or tiamazole 5, 10, 30 mg), and from the volatile thiouracyl (PTU
propylthiouracil 50,100 mg)
2. Thyroidectomy: new surgery is performed when the patient is euthyroid, clinical or
biochemical.
3. Radioactive iodine.
Prognosis
Dubia ad bonam. Mortality of thyroid crisis with adequate treatment is 10-15%.
Individuals with normal high-thyroid function tests, subclinical hyperthyroidism, and
clinical hyperthyroidism will increase the risk of atrial fibrillation. Hyperthyroidism is
also associated with an increased risk of heart failure (6% of patients), which may be
secondary to atrial fibrillation or tachycardia with dimediasicardiomyopathy. Heart
failure is usually reversible when hyperthyroidism is treated. Patients with
hyperthyroidism are also at risk for pulmonary hypertension secondary to increased
cardiac output and decreased pulmonary vascular resistance. In patients with pre-
existing heart disease, hyperthyroidism increases the risk of death (hazard ratio [HR]
= 1.57), and possibly even in patients without heart. It also increases the risk of
ischemic stroke (HR = 1.44) between adults 18 to 44 years. Untreated
hyperthyroidism also affects low bone mineral density and increases the risk of hip
fracture.
There are 3 treatment modalities that can be used: antithyroid drugs (ATDs),
radioactive iodine therapy and thyroidectomy. ATDs are suggested in GD patients
with the following conditions: a. Patients with high likelihood of remission (patients,
especially females, with mild disease, small goiters, and negative or low-titer TRAb)
b. Elderly or others with comorbidities increasing surgical risk or with limited life
expectancy c. Individuals in nursing homes or other care facilities who may have
limited longevity and are unable to follow radiation safety regulations d. Patients with
previously operated or irradiated necks e. Moderate-to-severe active Graves’
ophthalmopathy (GO) Radioactive iodine therapy is highly favored in GD patients
with the following clinical conditions: a. Females planning a pregnancy in the future
(in more than 4–6 months following radioiodine therapy, provided thyroid hormone
levels are normal), b. Individuals with comorbidities increasing surgical risk c.
Patients with previously operated or externally irradiated necks, or lack of access to
a high-volume thyroid surgeon d. Contraindications to ATDs use Surgical procedures
are recommended in patients with GD with the following conditions: a. Symptomatic
compression or large goiters (≥80 g) b. Relatively low uptake of radioactive iodine c.
When thyroid malignancy is documented or suspected (e.g., suspicious or
indeterminate cytology); d. Large nonfunctioning, photopenic or hypofunctioning
nodule e. Coexisting hyperparathyroidism requiring surgery f. Females planning a
pregnancy in <4–6 months (i.e., before thyroid hormone levels would be normal if
radioactive iodine were chosen as therapy), especially if TRAb levels are particularly
high g. Patients with moderate-to-severe active GO
Contraindications to a particular modality as treatment for Graves’
hyperthyroidism:
Prognosis
GD prognosis is well-reflected with remission and relapse rates.
Remission rates among adults are higher than children.
ATDs are able to induce permanent remission in 30-50% cases. If
relapse occurs in GD patients treated with ATDs, then destructive therapy is
more likely to be a more appropriate option. Following 12-18 months of ATDs
administration, approximately more than 50% of patients will develop a
relapse. Several studies reported that a high TSH-R Ab level prior to therapy
discontinuation suspectedly related to high relapse rate.
T3/T4 ratio of more than 20 is related to more than 80% relapse risk.
Low TSH level 4 weeks after ATDs discontinuation has been correlated with
relapse occurrence in 70% cases. There is a correlation between thyroid
volume and blood flow, in which this finding strengthened previous known
correlation between large struma and high risk to recur. Superior thyroid artery
blood flow also has already been known as one of relapse risk predictors.
All patients shall be strictly-monitored for relapse occurrence after
discontinuation of ATDs. Approximately 75% relapse events occurred in the
first 3 months after discontinuation. If relapse does occur, further ATDs
administration in a longer period shall be prescribed or destructive therapy is
likely to be considered.